1999
DOI: 10.1093/hmg/8.3.397
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Intranuclear inclusions and neuritic aggregates in transgenic mice expressing a mutant N-terminal fragment of huntingtin [published erratum appears in Hum Mol Genet 1999 May;8(5):943]

Abstract: Huntington's disease (HD) is an inherited, neurodegenerative disorder caused by the expansion of a glutamine repeat in the N-terminus of the huntingtin protein. To gain insight into the pathogenesis of HD, we generated transgenic mice that express a cDNA encoding an N-terminal fragment (171 amino acids) of huntingtin with 82, 44 or 18 glutamines. Mice expressing relatively low steady-state levels of N171 huntingtin with 82 glutamine repeats (N171-82Q) develop behavioral abnormalities, including loss of coordin… Show more

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Cited by 711 publications
(597 citation statements)
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“…Sequestration of mTOR to aggregates was associated with reduced amounts of soluble mTOR (relative to tubulin) in stable inducible cell lines expressing mutant versus wild-type huntingtin (Figs. 1d and 2a) and in brain lysates of mice expressing mutant huntingtin 16 (Fig. 2b) versus control littermates.…”
Section: Results Mtor Is Sequestered Into Huntingtin Aggregatesmentioning
confidence: 89%
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“…Sequestration of mTOR to aggregates was associated with reduced amounts of soluble mTOR (relative to tubulin) in stable inducible cell lines expressing mutant versus wild-type huntingtin (Figs. 1d and 2a) and in brain lysates of mice expressing mutant huntingtin 16 (Fig. 2b) versus control littermates.…”
Section: Results Mtor Is Sequestered Into Huntingtin Aggregatesmentioning
confidence: 89%
“…Sequestration of mTOR was not an artefact of protein overexpression or aggregation, as we found no colocalization of certain upstream mTOR regulators or unrelated proteins (Akt, Pdk1, Pten) with mutant huntingtin aggregates (data not shown). mTOR was also sequestered in huntingtin aggregates in brains of transgenic mice expressing N-terminal mutant huntingtin fragments 16 (Fig. 1b) and of individuals with Huntington disease (Fig.…”
Section: Results Mtor Is Sequestered Into Huntingtin Aggregatesmentioning
confidence: 95%
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“…The R6/1 and R6/2 lines, which express mutant human exon 1 HTT, were the first transgenic lines produced (Mangiarini et al, 1996) and the R6/2 mouse has been the most extensively studied and utilized mouse model of HD to date. Another N-terminal transgenic mouse is the N171-82Q line (Schilling et al, 1999) expressing a 171 amino acid mutant HTT fragment under the regulation of the mouse prion promoter, which directs expression primarily in the brain. These and other N-terminal transgenics are available from The Jackson Laboratory (JAX) and/or CHDI Foundation (Table 1).…”
Section: I1 N-terminal Transgenic Modelsmentioning
confidence: 99%